上海交通大学学报(医学版)2025,Vol.45Issue(10):1333-1341,9.DOI:10.3969/j.issn.1674-8115.2025.10.008
GRK调控M1乙酰胆碱受体偏向性结合下游信号转导蛋白的机制研究
Mechanism of GRK subtypes modulating the unique binding properties of M1 acetylcholine receptor and transducers
摘要
Abstract
Objective·To investigate the mechanisms by which different subtypes of G protein-coupled receptor kinases(GRKs)regulate the biased signaling transduction mediated by the muscarinic acetylcholine receptor 1(M1 receptor),focusing on their molecular effects in modulating the binding of the M1 receptor to the downstream heterotrimeric G protein(Gαq-Gβ1-Gγ2)andβ-arrestin 2(βarr2).Methods·By establishing a highly sensitive protein interaction detection system based on bioluminescence resonance energy transfer(BRET),six M1 receptor agonists/allosteric modulators were selected to measure the dynamic interactions between the M1 receptor and four GRK subtypes(GRK2/3/5/6),βarr2,and the G protein under stimulation.All BRET data were statistically quantified using the area under the curve(AUC)of the time-response curves.First,concentration-effect curves were established by treatment with gradient concentrations of agonists/allosteric modulators and AUC fitting,to comprehensively analyze the differences in efficacy between each agonist/allosteric modulator and the endogenous agonist acetylcholine chloride(ACh)in promoting the interactions of M1 receptor with GRK3/5,βarr2,and the G protein;next,GRKs were divided into two groups based on subtypes:GRK2/3 and GRK5/6.The maximum AUC values for the interaction between the M1 receptor and the two GRK groups under high concentrations were calculated respectively,to further evaluate the regulatory propensity of different types of GRKs on the binding strength of the M1 receptor to βarr2 or the G protein.Results·All six agonists/allosteric modulators effectively induced the association of the M1 receptor with GRK3,while simultaneousey inducing dissociation of the M1 receptor from GRK5.The allosteric modulator BQCA not only activated the M1 receptor alone and triggered its binding to downstream signaling proteins,but also,when co-treated with ACh,caused a significant leftward shift of the concentration-effect curves in the M1-G protein and M1-βarr2 systems,suggesting that its potentiation effect on ACh was mainly achieved by reducing the half-maximal effective concentration.A moderate positive correlation was observed between the maximum AUC values of M1-βarr2 and M1-G protein interactions induced by the seven groups of drug treatments(r=0.722,P=0.067).Further analysis showed that the ratio of the maximum AUC for M1-GRK2/3 interaction to that for M1-GRK5/6 interaction was also positively correlated with the ratio of the maximum AUC for M1-βarr2 interaction to that for M1-G protein interaction(r=0.760,P=0.047).Conclusion·The M1 receptor may be pre-coupled with GRK5/6 under basal conditions,and they dissociate upon receptor activation,suggesting that GRK5/6 may be involved in M1 receptor inactivation or signal reprogramming.The relative efficiency of the M1 receptor's interaction with different GRK subtypes determines its preference for downstream signaling pathways.关键词
毒蕈碱型乙酰胆碱受体1/G蛋白偶联受体激酶/G蛋白偶联受体/信号偏向性Key words
muscarinic acetylcholine receptor 1(M1 receptor)/G protein-coupled receptor kinase(GRK)/G protein-coupled receptor/signaling bias分类
医药卫生引用本文复制引用
魏嘉丽,王冬雪,王诗绮,徐见容,赵佩珅,赵兰雪..GRK调控M1乙酰胆碱受体偏向性结合下游信号转导蛋白的机制研究[J].上海交通大学学报(医学版),2025,45(10):1333-1341,9.基金项目
上海市高水平地方高校建设项目(ZXY24009) (ZXY24009)
国家级中医西医会聚创新平台建设[ZY(2025-2027)-2-2-1]. High-Level Local University Construction Project in Shanghai(ZXY24009) (2025-2027)
Three-year Action Plan for Shanghai TCM Development and Inheritance Program[ZY(2025‒2027)-2-2-1]. (2025‒2027)
